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Protein-binding effect

In experimental animals and in vitro, DHBs show a variety of biological effects including binding of metaboHtes to various proteins. Clastogenic effects have been observed in vitro and in some in vivo studies with the three compounds. No reproductive effects have been shown by conventional studies with either hydroquinone, catechol, or resorcinol (122). Hydroquinone has been shown to induce nephrotoxicity and kidney tumors at very high doses in some strains of rat (123) catechol induces glandular stomach tumors at very high dose (124). Repeated dermal appHcation of resorcinol did not induce cancer formation (125). [Pg.494]

Sulfaphenazole (684) and sulfazamet (685) are both examples of relatively short acting sulfonamides (B-80MI40406) and their antibacterial activity has been tested against Escherichia coli, the former being more effective than the latter. Sulfaphenazole also displaces sulfonyl ureas from protein binding sites on human serum albumin and consequently increases the concentration of the free (active) drug and produces a more intense reaction that may result in hypoglycemia. [Pg.291]

The way in which molecular chaperones interact with polypeptides during the folding process is not completely understood. What is clear is that chaperones bind effectively to the exposed hydrophobic regions of partially folded structures. These folding intermediates are less compact than the native folded proteins. They contain large amounts of secondary and even some tertiary... [Pg.192]

Triiodothyronine (3, 5,3-L-triiodothyronine, T3) is a thyroid hormone. It is producedby outer ring deiodination of thyroxine (T4) in peripheral tissues. The biologic activity of T3 is 3-8 times higher than that of T4. T3 is 99.7% protein-bound and is effective in its free non-protein-bound form. The half-life of triiodothyronine is about 19 h. The daily tur nover of T3 is 75%. Triiodothyronine acts via nuclear receptor binding with subsequent induction of protein synthesis. Effects of thyroid hormones are apparent in almost all organ systems. They include effects on the basal metabolic rate and the metabolisms of proteins, lipids and carbohydrates. [Pg.1243]

The activity of 4E is regulated in a second way, and this also involves phosphorylation. A recently discovered set of proteins bind to and inactivate 4E. These proteins include 4E-BP1 (BPl, also known as PHAS-1) and the closely related proteins 4E-BP2 and 4E-BP3. BPl binds with high affinity to 4E. The [4E] [BP1] association prevents 4E from binding to 4G (to form 4F). Since this interaction is essential for the binding of 4F to the ribosomal 40S subunit and for correctly positioning this on the capped mRNA, BP-1 effectively inhibits translation initiation. [Pg.367]

The administration of cloflbrate to a patient taking warfarin will potentiate the anticoagulant effect of warfarin by displacing It from Its protein binding site (7). This Interaction will cause... [Pg.277]

Casini, A., Cinellu, M.A., Minghetti, G., Gabbiani, C., Coronnello, M., Mini, E. and Messori, L. (2006) Structural and solution chemistry, antiproliferative effects, and DNA and protein binding properties of a series of dinudear gold(l II) compounds with bipyridyl ligands. Journal of Medicinal Chemistry, 49, 5524. [Pg.89]


See other pages where Protein-binding effect is mentioned: [Pg.472]    [Pg.139]    [Pg.100]    [Pg.312]    [Pg.11]    [Pg.2953]    [Pg.39]    [Pg.33]    [Pg.472]    [Pg.139]    [Pg.100]    [Pg.312]    [Pg.11]    [Pg.2953]    [Pg.39]    [Pg.33]    [Pg.547]    [Pg.256]    [Pg.259]    [Pg.463]    [Pg.181]    [Pg.2063]    [Pg.21]    [Pg.146]    [Pg.252]    [Pg.265]    [Pg.370]    [Pg.196]    [Pg.69]    [Pg.69]    [Pg.294]    [Pg.430]    [Pg.448]    [Pg.449]    [Pg.874]    [Pg.905]    [Pg.923]    [Pg.446]    [Pg.28]    [Pg.140]    [Pg.501]    [Pg.440]    [Pg.194]    [Pg.56]    [Pg.25]    [Pg.81]   
See also in sourсe #XX -- [ Pg.3031 , Pg.3032 ]




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